Test Directory
Hypophosphatasia (HPP) and Osteogenesis Imperfecta (OI) Genetic Panel
Justification
Specimen Requirements
| Sample Type | Volume Required | Minimum Volume | Stability | |
|---|---|---|---|---|
| PREFERRED | EDTA Whole Blood | 3mL | 1mL | Room Temp.: 1 month Refrigerated: 1 month |
| ALTERNATIVE | Cheek swab | 2 swab | - | Room Temp.: 1 month Refrigerated: 1 month |
| REJECTION CRITERIA | Sample contamination; sample compromised |
| SPECIAL INSTRUCTIONS | - |
General Information
| METHODOLOGY | NGS |
| STAT TAT | < 48 hours (M-F) |
| STAT TAT Performance | > 90% of results released in 48 hours |
| ROUTINE TAT | < 5 days (M-F) |
| ALTERNATIVE NAMES | HPP/OI Genetic Sequencing |
| DESCRIPTION | This test sequences the exons plus 20bp of the flanking introns from the following genes: ALPL/TNSALP, BMP1, COL1A1, COL1A2, CREB3L1, CRTAP, FKBP10, IFITM5, LEPRE1/P3H1, OSX/SP7, PLOD2, PPIB, SERPINF1, SERPINH1, TMEM38B, WNT1. Sanger sequencing may be used to confirm variants as needed. |
| LIMITATIONS | This test will not detect variants located outside of the targeted DNA regions. This test is not optimized to detect chimerism or somatic mosaicism. This test will detect small indels but may miss larger deletions or duplications. Balanced structural variants will not be detected unless specifically targeted by a custom PCR assay. |
| NORMAL RANGE | Interpretation: Negative |
| ASSOCIATED TESTING | - |
| REFERENCES | Taillandier A, et al. Molecular diagnosis of hypophosphatasia and differential diagnosis by targeted Next Generation Sequencing. Mol Genet Metab. 2015 Nov;116(3):215-20. Sabir AH, Cole T. The evolving therapeutic landscape of genetic skeletal disorders. Orphanet J Rare Dis. 2019 Dec 30;14(1):300. |
| SAMPLE REPORT | Upon request |
| NEW YORK STATE APPROVED | No |
Test Codes
| ORDER CODE | P1210 |
| CPT CODE | 81408x2, 81479x14 |
| LOINC CODE | 77084-2 |